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首页> 外文期刊>eLife journal >Malaria parasite LIMP protein regulates sporozoite gliding motility and infectivity in mosquito and mammalian hosts
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Malaria parasite LIMP protein regulates sporozoite gliding motility and infectivity in mosquito and mammalian hosts

机译:疟原虫LIMP蛋白调节蚊子和哺乳动物宿主中子孢子的滑行运动和感染性

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Gliding motility allows malaria parasites to migrate and invade tissues and cells in different hosts. It requires parasite surface proteins to provide attachment to host cells and extracellular matrices. Here, we identify the Plasmodium protein LIMP (the name refers to a gliding phenotype in the sporozoite arising from epitope tagging of the endogenous protein) as a key regulator for adhesion during gliding motility in the rodent malaria model P. berghei. Transcribed in gametocytes, LIMP is translated in the ookinete from maternal mRNA, and later in the sporozoite. The absence of LIMP reduces initial mosquito infection by 50%, impedes salivary gland invasion 10-fold, and causes a complete absence of liver invasion as mutants fail to attach to host cells. GFP tagging of LIMP caused a limping defect during movement with reduced speed and transient curvature changes of the parasite. LIMP is an essential motility and invasion factor necessary for malaria transmission.
机译:滑行运动使疟原虫能够迁移并侵入不同宿主中的组织和细胞。它需要寄生虫表面蛋白来提供对宿主细胞和细胞外基质的附着。在这里,我们确定疟原虫蛋白LIMP(名称是指子孢子中内源蛋白表位标记引起的滑动表型),作为啮齿类疟疾模型伯氏疟原虫滑行运动过程中粘附的关键调节剂。 LIMP在配子细胞中转录,从母体mRNA的子代翻译为子代子,随后在子孢子中翻译。 LIMP的缺失可将最初的蚊子感染减少50%,阻止唾液腺侵袭10倍,并且由于突变体无法附着在宿主细胞上而导致肝脏的完全侵袭。 LIMP的GFP标签在运动过程中引起lim行缺陷,其速度降低且寄生虫的瞬时曲率发生了变化。 LIMP是传播疟疾所必需的基本动力和入侵因子。

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